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增强对受与良好临床结果相关的HLA I类等位基因限制的HIV-1隐蔽表位的识别。

Enhanced Recognition of HIV-1 Cryptic Epitopes Restricted by HLA Class I Alleles Associated With a Favorable Clinical Outcome.

作者信息

Bansal Anju, Mann Tiffanie, Sterrett Sarah, Peng Binghao J, Bet Anne, Carlson Jonathan M, Goepfert Paul A

机构信息

*Department of Medicine, University of Alabama at Birmingham, Birmingham, AL; and †Microsoft Research, Redmond, WA.

出版信息

J Acquir Immune Defic Syndr. 2015 Sep 1;70(1):1-8. doi: 10.1097/QAI.0000000000000700.

DOI:10.1097/QAI.0000000000000700
PMID:26322665
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4556167/
Abstract

BACKGROUND

Cryptic epitopes (CEs) are peptides derived from the translation of 1 or more of the 5 alternative reading frames (ARFs; 2 sense and 3 antisense) of genes. Here, we compared response rates to HIV-1-specific CE predicted to be restricted by HLA-I alleles associated with protection against disease progression to those without any such association.

METHODS

Peptides (9mer to 11mer) were designed based on HLA-I-binding algorithms for B27, B57, or B5801 (protective alleles) and HLA-B5301 or B*5501 (nonprotective allele) in all 5 ARFs of the 9 HIV-1 encoded proteins. Peptides with >50% probability of being an epitope (n = 231) were tested for T-cell responses in an IFN-γ enzyme-linked immunosorbent spot (ELISpot) assay. Peripheral blood mononuclear cell samples from HIV-1 seronegative donors (n = 42) and HIV-1 seropositive patients with chronic clade B infections (n = 129) were used.

RESULTS

Overall, 16%, 2%, and 2% of chronic HIV infected patients had CE responses by IFN-γ ELISpot in the protective, nonprotective, and seronegative groups, respectively (P = 0.009, Fischer exact test). Twenty novel CE-specific responses were mapped (median magnitude of 95 spot forming cells/10 peripheral blood mononuclear cells), and most were both antisense derived (90%) and represented ARFs of accessory proteins (55%). CE-specific CD8 T cells were multifunctional and proliferated when assessed by intracellular cytokine staining.

CONCLUSIONS

CE responses were preferentially restricted by the protective HLA-I alleles in HIV-1 infection, suggesting that they may contribute to viral control in this group of patients.

摘要

背景

隐蔽表位(CEs)是源自基因5个可变阅读框(ARFs;2个正义和3个反义)中1个或更多个的翻译产物的肽段。在此,我们比较了针对预测受与预防疾病进展相关的HLA - I等位基因限制的HIV - 1特异性CE的反应率与那些无此类关联的反应率。

方法

基于HLA - I结合算法,针对9种HIV - 1编码蛋白的所有5个ARFs中的B27、B57或B5801(保护性等位基因)以及HLA - B5301或B*5501(非保护性等位基因)设计肽段(9聚体至11聚体)。对具有>50%表位可能性的肽段(n = 231)进行γ干扰素酶联免疫斑点(ELISpot)试验以检测T细胞反应。使用来自HIV - 1血清阴性供体(n = 42)和慢性B亚型感染的HIV - 1血清阳性患者(n = 129)的外周血单个核细胞样本。

结果

总体而言,慢性HIV感染患者中,分别有16%、2%和2%在保护性、非保护性和血清阴性组中通过γ干扰素ELISpot检测到CE反应(P = 0.009,Fisher精确检验)。绘制了20种新的CE特异性反应图谱(中位数强度为95个斑点形成细胞/10个外周血单个核细胞),并且大多数反应源自反义序列(90%)且代表辅助蛋白的ARFs(55%)。通过细胞内细胞因子染色评估时,CE特异性CD8 T细胞具有多功能性且能增殖。

结论

在HIV - 1感染中,CE反应优先受保护性HLA - I等位基因限制,表明它们可能有助于这组患者的病毒控制。